Estimated impact of maternal vaccination on global paediatric influenza-related in-hospital mortality: A retrospective case series

eClinicalMedicine, Volume 37, Year 2021

Ukuhunyushwa

Background: Influenza virus infection is an important cause of under-five mortality. Maternal vaccination protects children younger than 3 months of age from influenza infection. However, it is unknown to what extent paediatric influenza-related mortality may be prevented by a maternal vaccine since global age-stratified mortality data are lacking. Methods: We invited clinicians and researchers to share clinical and demographic characteristics from children younger than 5 years who died with laboratory-confirmed influenza infection between January 1, 1995 and March 31, 2020. We evaluated the potential impact of maternal vaccination by estimating the number of children younger than 3 months with in-hospital influenza-related death using published global mortality estimates. Findings: We included 314 children from 31 countries. Comorbidities were present in 166 (53%) children and 41 (13%) children were born prematurely. Median age at death was 8·6 (IQR 4·5–16·6), 11·5 (IQR 4·3–24·0), and 15·5 (IQR 7·4–27·0) months for children from low- and lower-middle-income countries (LMICs), upper-middle-income countries (UMICs), and high-income countries (HICs), respectively. The proportion of children younger than 3 months at time of death was 17% in LMICs, 12% in UMICs, and 7% in HICs. We estimated that 3339 annual influenza-related in-hospital deaths occur in the first 3 months of life globally. Interpretation: In our study, less than 20% of children is younger than 3 months at time of influenza-related death. Although maternal influenza vaccination may impact maternal and infant influenza disease burden, additional immunisation strategies are needed to prevent global influenza-related childhood mortality. The missing data, global coverage, and data quality in this study should be taken into consideration for further interpretation of the results. Funding: Bill & Melinda Gates Foundation. The FLU GOLD study was initiated in October 2017. We invited our existing global respiratory syncytial virus (RSV) GOLD network [15], consisting of individual investigators, research groups, and clinicians, to share individual-level data of children aged 0–59 months who had died with laboratory-confirmed influenza infection between January 1, 1995 and March 31, 2020. YNL, NIM, FSV, and LJB had full access to all the data in the study. We excluded community deaths due to limited available data (n = 8) and children with influenza-related mortality after stem cell transplantation. Additionally, we searched the literature using PubMed for “influenza” combined with “death”, “deaths”, “died”, “mortality”, “fatality”, or “case fatality ratio (CFR)” and “pediatric”, “pediatrics”, “child”, or “children” and invited authors to share additional (unpublished) cases. Collaborators were invited to share data between October 13, 2017, and March 31, 2020 through a link to a questionnaire (Supplementary Material) in Research Online, an electronic data capture platform [16]. We collected demographic and clinical characteristics and compared these between children from different income groups. Countries of origin were categorised as LMIC (LIC and LMIC combined), upper-middle-income countries (UMIC), and HIC according to the World Bank classifications for 2020 [17]. We compared age distribution at time of death for the 3 income groups and between the following 3 patient populations: children with comorbidities, healthy term children, and healthy preterm children (without comorbidities). A comorbidity was defined as at least one underlying disease, such as congenital heart disease, chronic lung disease or a genetic disorder. Prematurity was defined as gestational age less than 37 weeks. If data for comorbidities or prematurity were not reported, we assumed that the children were healthy term. We calculated weight-for-age z-scores as previously described [15]. We determined the proportion of children who died within the influenza virus epidemic season by comparing age at death and seasonality within the country of origin as estimated by a recent systematic analysis on global patterns of monthly influenza virus activity [18]. We compared the proportion of in-hospital deaths under 6 months of age in our study to the proportions from published studies used for the recent global influenza burden study from the Respiratory Virus Global Epidemiology Network [1]. We calculated age at influenza infection by subtracting the number of days between onset of influenza-related symptoms and influenza-related death from age at influenza-related death. We then determined the proportion of children under 3 months of age at time of influenza infection. We differentiated between children with community-acquired and hospital-acquired influenza infection. In case the setting where influenza had been acquired was not provided, and if there were no strong indications of nosocomial infection based on timeframe and clinical disease course, we assumed the infection had been community-acquired. We assumed that deaths occurred within the hospital if data on location of death were missing. To evaluate the minimum expected impact of maternal vaccination on influenza-related deaths assuming 100% vaccine efficacy and complete vaccination coverage, we multiplied the proportion of children younger than 3 months at time of community-acquired in-hospital death by the estimated total number of global influenza-associated ALRI in-hospital deaths under 5 years of age for each World Bank income group [1]. We compared demographic and clinical characteristics between different income groups, excluding cases with missing data for comorbidities or prematurity. We performed subgroup analyses and compared characteristics for children with hospital-acquired and community-acquired influenza-related death. Furthermore, we differentiated between seasonal and pandemic influenza-related deaths by excluding children with influenza A(H1N1)pdm09 who died within the timeframe of the WHO-declared pandemic (June 2009 – August 2010) from the analyses. Lastly, we analysed to what extent our results were sensitive to the contribution of a large number of cases from Ecuador, United Kingdom, Kenya, Turkey and South Africa (n = 145) by excluding these countries from our analyses. Since de-identified secondary patient data were used in the FLU GOLD study, parental informed consent was waived by the institutional research board of the University Medical Centre Utrecht. Ethical approval was obtained for individual collaborating institutes when required. We report descriptive statistics for all variables. Continuous variables are presented as median with interquartile ranges (IQR). Categorical variables are presented as frequencies and proportions. We used the χ2-test or the Fisher’s exact test to determine statistical significance between groups for categorical parameters. We report conservative exact p values instead of asymptotic p values because of the small sample size. The Mann-Whitney U test was used for all continuous parameters. We applied the Bonferroni correction for multiple testing between World Bank income groups. All statistical analyses were performed with SPSS (version 21·0; IBM Corp, Armonk, NY). The funder had no role in study design, data collection, data analysis, data interpretation, writing of the report, or the decision to submit the paper for publication. YNL, NIM, FSV, and LJB had full access to all the data in the study and NIM had final responsibility for the decision to submit for publication.

I-AI Digest

Study Justification:

The study titled “Estimated impact of maternal vaccination on global paediatric influenza-related in-hospital mortality: A retrospective case series” aims to investigate the potential impact of maternal vaccination on reducing influenza-related deaths in children under the age of 3 months. This is important because influenza virus infection is a significant cause of mortality in children under the age of five. Understanding the potential benefits of maternal vaccination can help inform public health strategies to reduce childhood mortality.

Highlights:

– The study included data from 314 children from 31 countries who died with laboratory-confirmed influenza infection.
– Comorbidities were present in 53% of the children, and 13% were born prematurely.
– The median age at death was 8.6 months for children from low- and lower-middle-income countries, 11.5 months for children from upper-middle-income countries, and 15.5 months for children from high-income countries.
– The proportion of children under 3 months at the time of death was 17% in low- and lower-middle-income countries, 12% in upper-middle-income countries, and 7% in high-income countries.
– The study estimated that globally, 3339 annual influenza-related in-hospital deaths occur in the first 3 months of life.

Recommendations:

– Maternal influenza vaccination may have an impact on reducing maternal and infant influenza disease burden.
– Additional immunization strategies are needed to prevent global influenza-related childhood mortality.
– Further interpretation of the results should consider the missing data, global coverage, and data quality in this study.

Key Role Players:

– Researchers and clinicians: To continue collecting and analyzing data on influenza-related deaths in children.
– Public health officials: To develop and implement immunization strategies, including maternal vaccination, to reduce childhood mortality.
– Healthcare providers: To promote and administer influenza vaccinations to pregnant women and infants.
– Policy makers: To allocate resources and support initiatives aimed at reducing influenza-related childhood mortality.

Cost Items for Planning Recommendations:

– Research and data collection: Funding for data collection, analysis, and publication of findings.
– Immunization programs: Budget for the development, production, and distribution of influenza vaccines for pregnant women and infants.
– Healthcare infrastructure: Investment in healthcare facilities and personnel to support vaccination efforts and provide healthcare services to pregnant women and infants.
– Public awareness campaigns: Funding for educational campaigns to raise awareness about the importance of influenza vaccination for pregnant women and infants.
Please note that the cost items provided are general categories and not actual cost estimates. The actual costs will vary depending on the specific context and implementation strategies.

Amandla Obufakazi

The strength of evidence for this abstract is 7 out of 10.
The evidence in the abstract is moderately strong. The study includes data from 314 children from 31 countries and provides estimates of influenza-related in-hospital deaths in children under 3 months of age. However, the study acknowledges missing data, limited global coverage, and data quality issues. To improve the strength of the evidence, the study could aim for a larger sample size, ensure comprehensive data collection, and include a more diverse range of countries. Additionally, conducting further analyses to validate the estimates and considering the limitations in the interpretation of the results would enhance the evidence.

Abstract

The FLU GOLD study was initiated in October 2017. We invited our existing global respiratory syncytial virus (RSV) GOLD network [15], consisting of individual investigators, research groups, and clinicians, to share individual-level data of children aged 0–59 months who had died with laboratory-confirmed influenza infection between January 1, 1995 and March 31, 2020. YNL, NIM, FSV, and LJB had full access to all the data in the study. We excluded community deaths due to limited available data (n = 8) and children with influenza-related mortality after stem cell transplantation. Additionally, we searched the literature using PubMed for “influenza” combined with “death”, “deaths”, “died”, “mortality”, “fatality”, or “case fatality ratio (CFR)” and “pediatric”, “pediatrics”, “child”, or “children” and invited authors to share additional (unpublished) cases. Collaborators were invited to share data between October 13, 2017, and March 31, 2020 through a link to a questionnaire (Supplementary Material) in Research Online, an electronic data capture platform [16]. We collected demographic and clinical characteristics and compared these between children from different income groups. Countries of origin were categorised as LMIC (LIC and LMIC combined), upper-middle-income countries (UMIC), and HIC according to the World Bank classifications for 2020 [17]. We compared age distribution at time of death for the 3 income groups and between the following 3 patient populations: children with comorbidities, healthy term children, and healthy preterm children (without comorbidities). A comorbidity was defined as at least one underlying disease, such as congenital heart disease, chronic lung disease or a genetic disorder. Prematurity was defined as gestational age less than 37 weeks. If data for comorbidities or prematurity were not reported, we assumed that the children were healthy term. We calculated weight-for-age z-scores as previously described [15]. We determined the proportion of children who died within the influenza virus epidemic season by comparing age at death and seasonality within the country of origin as estimated by a recent systematic analysis on global patterns of monthly influenza virus activity [18]. We compared the proportion of in-hospital deaths under 6 months of age in our study to the proportions from published studies used for the recent global influenza burden study from the Respiratory Virus Global Epidemiology Network [1]. We calculated age at influenza infection by subtracting the number of days between onset of influenza-related symptoms and influenza-related death from age at influenza-related death. We then determined the proportion of children under 3 months of age at time of influenza infection. We differentiated between children with community-acquired and hospital-acquired influenza infection. In case the setting where influenza had been acquired was not provided, and if there were no strong indications of nosocomial infection based on timeframe and clinical disease course, we assumed the infection had been community-acquired. We assumed that deaths occurred within the hospital if data on location of death were missing. To evaluate the minimum expected impact of maternal vaccination on influenza-related deaths assuming 100% vaccine efficacy and complete vaccination coverage, we multiplied the proportion of children younger than 3 months at time of community-acquired in-hospital death by the estimated total number of global influenza-associated ALRI in-hospital deaths under 5 years of age for each World Bank income group [1]. We compared demographic and clinical characteristics between different income groups, excluding cases with missing data for comorbidities or prematurity. We performed subgroup analyses and compared characteristics for children with hospital-acquired and community-acquired influenza-related death. Furthermore, we differentiated between seasonal and pandemic influenza-related deaths by excluding children with influenza A(H1N1)pdm09 who died within the timeframe of the WHO-declared pandemic (June 2009 – August 2010) from the analyses. Lastly, we analysed to what extent our results were sensitive to the contribution of a large number of cases from Ecuador, United Kingdom, Kenya, Turkey and South Africa (n = 145) by excluding these countries from our analyses. Since de-identified secondary patient data were used in the FLU GOLD study, parental informed consent was waived by the institutional research board of the University Medical Centre Utrecht. Ethical approval was obtained for individual collaborating institutes when required. We report descriptive statistics for all variables. Continuous variables are presented as median with interquartile ranges (IQR). Categorical variables are presented as frequencies and proportions. We used the χ2-test or the Fisher’s exact test to determine statistical significance between groups for categorical parameters. We report conservative exact p values instead of asymptotic p values because of the small sample size. The Mann-Whitney U test was used for all continuous parameters. We applied the Bonferroni correction for multiple testing between World Bank income groups. All statistical analyses were performed with SPSS (version 21·0; IBM Corp, Armonk, NY). The funder had no role in study design, data collection, data analysis, data interpretation, writing of the report, or the decision to submit the paper for publication. YNL, NIM, FSV, and LJB had full access to all the data in the study and NIM had final responsibility for the decision to submit for publication.

Izinto zokwakha

https://efashare.b-cdn.net/materials/14cc34b62256e36efce08662e038e8a36df5d4f233d6f00eefa8d4abaf56045c/mmc1.docx

Emisha

Based on the provided information, it seems that the study is focused on estimating the impact of maternal vaccination on global pediatric influenza-related in-hospital mortality. The study aims to evaluate the potential benefits of maternal influenza vaccination in preventing influenza-related deaths in children under 3 months of age.

To improve access to maternal health and address the issue of pediatric influenza-related mortality, the following innovations could be considered:

1. Maternal Influenza Vaccination Programs: Implementing vaccination programs specifically targeting pregnant women to increase their immunity against influenza and reduce the risk of transmission to their infants.

2. Education and Awareness Campaigns: Conducting educational campaigns to raise awareness among pregnant women and healthcare providers about the importance of maternal influenza vaccination and its potential benefits in preventing influenza-related deaths in infants.

3. Strengthening Healthcare Infrastructure: Improving healthcare infrastructure, especially in low- and middle-income countries, to ensure access to maternal healthcare services, including vaccination, antenatal care, and postnatal care.

4. Integration of Vaccination Services: Integrating maternal influenza vaccination services with existing antenatal care programs to ensure that pregnant women receive the vaccine as part of routine care.

5. Mobile Health (mHealth) Solutions: Utilizing mobile health technologies to provide information, reminders, and appointment scheduling for maternal influenza vaccination, making it more accessible and convenient for pregnant women.

6. Public-Private Partnerships: Collaborating with private sector organizations, such as pharmaceutical companies and non-profit organizations, to support maternal influenza vaccination programs and improve access to vaccines in resource-limited settings.

7. Research and Data Collection: Conducting further research and data collection to better understand the impact of maternal influenza vaccination on pediatric influenza-related mortality, especially in different income groups and geographical regions.

These innovations can contribute to improving access to maternal health and reducing pediatric influenza-related mortality by increasing vaccination rates among pregnant women and ensuring that infants are protected from influenza infection during the vulnerable early months of life.

AI Innovations Description

The recommendation that can be developed into an innovation to improve access to maternal health based on the provided information is to implement maternal influenza vaccination programs. The study suggests that maternal vaccination can protect children younger than 3 months from influenza infection, which is a significant cause of under-five mortality. By vaccinating pregnant women against influenza, it is possible to reduce the risk of influenza-related deaths in infants. This innovation would require the establishment of vaccination programs targeting pregnant women, ensuring widespread access to the vaccine, and raising awareness among healthcare providers and pregnant women about the importance of maternal influenza vaccination. By implementing such programs, it is possible to prevent global influenza-related childhood mortality and improve maternal and infant health outcomes.

AI Innovations Methodology

The study you provided, titled “Estimated impact of maternal vaccination on global pediatric influenza-related in-hospital mortality: A retrospective case series,” aims to assess the potential impact of maternal vaccination on reducing pediatric influenza-related deaths. The methodology used in the study involves collecting individual-level data of children aged 0-59 months who died with laboratory-confirmed influenza infection between January 1, 1995, and March 31, 2020.

Here is a brief summary of the methodology used in the study:

1. Data Collection: The study invited clinicians, researchers, and collaborators to share clinical and demographic characteristics of children who died with laboratory-confirmed influenza infection. Existing global respiratory syncytial virus (RSV) GOLD network data were also utilized.

2. Exclusion Criteria: Community deaths with limited available data and children with influenza-related mortality after stem cell transplantation were excluded from the analysis.

3. Literature Search: The study conducted a literature search using PubMed to identify additional cases of pediatric influenza-related deaths. Authors were invited to share any unpublished cases.

4. Data Analysis: Demographic and clinical characteristics were collected and compared between children from different income groups (low- and lower-middle-income countries, upper-middle-income countries, and high-income countries). Age distribution at the time of death was compared among different patient populations (children with comorbidities, healthy term children, and healthy preterm children).

5. Estimation of Influenza-related Deaths: The study estimated the number of children younger than 3 months with in-hospital influenza-related death using published global mortality estimates. The impact of maternal vaccination was evaluated by calculating the minimum expected impact assuming 100% vaccine efficacy and complete vaccination coverage.

6. Statistical Analysis: Descriptive statistics, including median with interquartile ranges (IQR) for continuous variables and frequencies/proportions for categorical variables, were used. Statistical tests such as the chi-square test, Fisher’s exact test, and Mann-Whitney U test were applied to determine significance.

7. Ethical Considerations: Parental informed consent was waived by the institutional research board, and ethical approval was obtained for individual collaborating institutes when required.

It is important to note that the study acknowledges the limitations of missing data, global coverage, and data quality, which should be considered when interpreting the results.

Overall, this study provides insights into the potential impact of maternal vaccination on reducing pediatric influenza-related deaths and highlights the need for additional immunization strategies to prevent global influenza-related childhood mortality.

Umbhali

Dima Health

Statistics:

Citations: 2

Identifiers:

DOI: 10.1016/j.eclinm.2021.100945

Research Areas:

Community Interventions, Genetics and Genomics, Health System and Policy, Maternal and Child Health, Noncommunicable Diseases, Social Determinants

Study Countries:

Kenya, Multi-Countries, South Africa

Study Design:

Cohort Study, Cross Sectional Study, Grounded Theory

Study Approach:

Mixed-methods, Quantitative, Systematic Review

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